IL-17 stimulates intraperitoneal neutrophil infiltration through the release of GROα chemokine from mesothelial cells

J Witowski, K Pawlaczyk, A Breborowicz… - The Journal of …, 2000 - journals.aai.org
J Witowski, K Pawlaczyk, A Breborowicz, A Scheuren, M Kuzlan-Pawlaczyk, J Wisniewska…
The Journal of Immunology, 2000journals.aai.org
IL-17 is a newly discovered cytokine implicated in the regulation of hemopoiesis and
inflammation. Because IL-17 production is restricted to activated T lymphocytes, the effects
exerted by IL-17 may help one to understand the contribution of T cells to the inflammatory
response. We investigated the role of IL-17 in leukocyte recruitment into the peritoneal
cavity. Leukocyte infiltration in vivo was assessed in BALB/Cj mice. Effects of IL-17 on
chemokine generation in vitro were examined in human peritoneal mesothelial cells …
Abstract
IL-17 is a newly discovered cytokine implicated in the regulation of hemopoiesis and inflammation. Because IL-17 production is restricted to activated T lymphocytes, the effects exerted by IL-17 may help one to understand the contribution of T cells to the inflammatory response. We investigated the role of IL-17 in leukocyte recruitment into the peritoneal cavity. Leukocyte infiltration in vivo was assessed in BALB/Cj mice. Effects of IL-17 on chemokine generation in vitro were examined in human peritoneal mesothelial cells (HPMC). Administration of IL-17 ip resulted in a selective recruitment of neutrophils into the peritoneum and increased levels of KC chemokine (murine homologue of human growth-related oncogene α (GROα). Pretreatment with anti-KC Ab significantly reduced the IL-17-driven neutrophil accumulation. Primary cultures of HPMC expressed IL-17 receptor mRNA. Exposure of HPMC to IL-17 led to a dose-and time-dependent induction of GROα mRNA and protein. Combination of IL-17 together with TNF-α resulted in an increased stability of GROα mRNA and synergistic release of GROα protein. Anti-IL-17 Ab blocked the effects of IL-17 in vitro and in vivo. IL-17 is capable of selectively recruiting neutrophils into the peritoneal cavity via the release of neutrophil-specific chemokines from the peritoneal mesothelium.
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